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Weight Loss Results in Increased Expression of Anti‐Inflammatory Protein CRISPLD2 in Mouse Adipose Tissue

机译:减肥导致小鼠脂肪组织中抗炎蛋白脆蛋白脆蛋白脆蛋白脆的表达增加

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摘要

Objective Obesity is a major risk factor for cardiovascular disease, metabolic syndrome, and type 2 diabetes mellitus, whereas weight loss is associated with improved health outcomes. It is therefore important to learn how adipose contraction during weight loss contributes to improved health. It was hypothesized that adipose tissue undergoing weight loss would have a unique transcriptomic profile, expressing specific genes that might improve health. Methods This study conducted an?RNA‐sequencing analysis of the epididymal adipose tissue of mice fed either a high‐fat diet (HFD) or a regular rodent chow diet (RD) ad libitum for 10 weeks versus a cohort of mice fed HFD for the first 5 weeks before being swapped to an RD for the remainder of the study (swapped diet [SWAP]). Results The swapped diet resulted in weight loss, with a parallel improvement in insulin sensitivity. RNA?sequencing revealed several transcriptomic signatures distinct to adipose tissue in SWAP mice, distinguished from both RD and HFD adipose tissue. The analysis found a unique upregulated mRNA that encodes a secreted lipopolysaccharide‐binding glycoprotein (CRISPLD2) in adipose tissue. Whereas cellular CRISPLD2 protein levels were unchanged, plasma CRIPSLD2 levels increased in SWAP mice following weight loss and could correlate with insulin sensitivity. Conclusions Taken together, these?data demonstrate that CRISPLD2 is a circulating adipokine that may regulate adipocyte remodeling during weight loss.
机译:客观肥胖是心血管疾病,代谢综合征和2型糖尿病的主要危险因素,而体重减轻与改善的健康结果有关。因此,重要的是要了解减肥期间的脂肪收缩有助于改善健康。假设脂肪组织接受体重减轻将具有独特的转录组型材,表达可能改善健康的特定基因。方法本研究进行了喂养高脂饮食(HFD)或常规啮齿动物味道饮食(RD)AD Libitum的对小鼠的附睾脂肪组织的RNA测序分析10周与喂养HFD的小鼠队列前5周前5周换成该研究剩余时间(交换饮食[Swap])。结果交换饮食导致体重减轻,胰岛素敏感性平行提高。 RNA?测序揭示了几种转发组签名,不同于伴随小鼠的脂肪组织,与RD和HFD脂肪组织不同。该分析发现了一种独特的上调MRNA,其在脂肪组织中编码分泌的脂多糖结合的糖蛋白(脆皮2)。虽然细胞脆蛋白水平不变,但在减肥后,血浆克劳斯德2水平增加,并且可以与胰岛素敏感性相关。结论在一起,这些呢?数据表明Cisspld2是循环adipokine,其可以在体重减轻期间调节脂肪细胞重塑。

著录项

  • 来源
    《Obesity》 |2019年第12期|共12页
  • 作者单位

    Department of Biochemistry and Molecular BiologyUniversity of Oklahoma Health Sciences;

    Department of Biochemistry and Molecular BiologyUniversity of Oklahoma Health Sciences;

    Department of PediatricsUniversity of Oklahoma Health Sciences CenterOklahoma City Oklahoma USA;

    Department of PediatricsUniversity of Oklahoma Health Sciences CenterOklahoma City Oklahoma USA;

    Department of PhysiologyUniversity of Oklahoma Health Sciences CenterOklahoma City Oklahoma USA;

    Department of Biochemistry and Molecular BiologyUniversity of Oklahoma Health Sciences;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 内分泌腺疾病及代谢病;
  • 关键词

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